Acute mTOR inhibition induces insulin resistance and alters substrate utilization in vivo
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Acute mTOR inhibition induces insulin resistance and alters substrate utilization in vivo. / Kleinert, Maximilian; Sylow, Lykke; Fazakerley, Daniel J.; Krycer, James R.; Thomas, Kristen C; Oxbøll, Anne-Julie; Jordy, Andreas Børsting; Jensen, Thomas Elbenhardt; Yang, Guang; Schjerling, Peter; Kiens, Bente; James, David E; Ruegg, Markus A; Richter, Erik A.
In: Molecular Metabolism, Vol. 3, No. 6, 2014, p. 630-641.Research output: Contribution to journal › Journal article › Research › peer-review
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TY - JOUR
T1 - Acute mTOR inhibition induces insulin resistance and alters substrate utilization in vivo
AU - Kleinert, Maximilian
AU - Sylow, Lykke
AU - Fazakerley, Daniel J.
AU - Krycer, James R.
AU - Thomas, Kristen C
AU - Oxbøll, Anne-Julie
AU - Jordy, Andreas Børsting
AU - Jensen, Thomas Elbenhardt
AU - Yang, Guang
AU - Schjerling, Peter
AU - Kiens, Bente
AU - James, David E
AU - Ruegg, Markus A
AU - Richter, Erik A.
N1 - CURIS 2014 NEXS 256
PY - 2014
Y1 - 2014
N2 - The effect of acute inhibition of both mTORC1 and mTORC2 on metabolism is unknown. A single injection of the mTOR kinase inhibitor, AZD8055, induced a transient, yet marked increase in fat oxidation and insulin resistance in mice, whereas the mTORC1 inhibitor rapamycin had no effect. AZD8055, but not rapamycin reduced insulin-stimulated glucose uptake into incubated muscles, despite normal GLUT4 translocation in muscle cells. AZD8055 inhibited glycolysis in MEF cells. Abrogation of mTORC2 activity by SIN1 deletion impaired glycolysis and AZD8055 had no effect in SIN1 KO MEFs. Re-expression of wildtype SIN1 rescued glycolysis. Glucose intolerance following AZD8055 administration was absent in mice lacking the mTORC2 subunit Rictor in muscle, and in vivo glucose uptake into Rictor-deficient muscle was reduced despite normal Akt activity. Taken together, acute mTOR inhibition is detrimental to glucose homeostasis in part by blocking muscle mTORC2, indicating its importance in muscle metabolism in vivo.
AB - The effect of acute inhibition of both mTORC1 and mTORC2 on metabolism is unknown. A single injection of the mTOR kinase inhibitor, AZD8055, induced a transient, yet marked increase in fat oxidation and insulin resistance in mice, whereas the mTORC1 inhibitor rapamycin had no effect. AZD8055, but not rapamycin reduced insulin-stimulated glucose uptake into incubated muscles, despite normal GLUT4 translocation in muscle cells. AZD8055 inhibited glycolysis in MEF cells. Abrogation of mTORC2 activity by SIN1 deletion impaired glycolysis and AZD8055 had no effect in SIN1 KO MEFs. Re-expression of wildtype SIN1 rescued glycolysis. Glucose intolerance following AZD8055 administration was absent in mice lacking the mTORC2 subunit Rictor in muscle, and in vivo glucose uptake into Rictor-deficient muscle was reduced despite normal Akt activity. Taken together, acute mTOR inhibition is detrimental to glucose homeostasis in part by blocking muscle mTORC2, indicating its importance in muscle metabolism in vivo.
U2 - 10.1060/j.molmet.2014.06.004
DO - 10.1060/j.molmet.2014.06.004
M3 - Journal article
VL - 3
SP - 630
EP - 641
JO - Molecular Metabolism
JF - Molecular Metabolism
SN - 2212-8778
IS - 6
ER -
ID: 123235528